doCRMAv1: Estimation and assessment of raw copy numbers at the single locus level (CRMA v1)
Description
Estimation and assessment of raw copy numbers at the single locus level (CRMA v1) based on [1].
The algorithm is processed in bounded memory, meaning virtually
any number of arrays can be analyzed on also very limited computer
systems.
Usage
"doCRMAv1"(csR, shift=+300, combineAlleles=TRUE, lengthRange=NULL, arrays=NULL, drop=TRUE, verbose=FALSE, ...) "doCRMAv1"(dataSet, ..., verbose=FALSE) "doASCRMAv1"(...)
Arguments
shift
An tuning parameter specifying how much to shift the
probe signals before probe summarization.
combineAlleles
A logical specifying whether allele probe pairs
should be summed before modelling or not. arrays
A integer vector specifying the subset of arrays
to process. If NULL, all arrays are considered. drop
If TRUE, the summaries are returned, otherwise
a named list of all intermediate and final results. ...
Additional arguments used to set up AffymetrixCelSet (when argument dataSet is specified). Allele-specific or only total-SNP signals
If you wish to obtain allele-specific estimates for SNPs, which
are needed to call genotypes or infer parent-specific copy numbers,
then use argument combineAlleles=FALSE. Total copy number
signals are still available.
If you know for certain that you will not use allele-specific
estimates, you will get slightly less noisy signals
(very small difference) if you use combineAlleles=TRUE. doASCRMAv1(...) is a wrapper for
doCRMAv1(..., combineAlleles=FALSE).References
[1] H. Bengtsson, R. Irizarry, B. Carvalho & T.P. Speed.
Estimation and assessment of raw copy numbers at the
single locus level,
Bioinformatics, 2008.
See Also
For CRMA v2 (recommended by authors), which is a single-array
improvement over CRMA v1, see doCRMAv2().